DE3884081T2 - Anti-acne composition. - Google Patents

Abstract

A hydroalcoholic solution with pH 2-3.5 of salicylic acid and an anionic taurate surfactant selected from the group consisting of sodium methyl cocoyl taurate and sodium methyl oleoyl taurate for the treatment of acne, is cosmetically acceptable, and results in the deposition of substantial amounts of salicylic acid into the stratum corneum with minimal penetration through the skin.

Description

The present invention relates to improved cosmetically acceptable compositions for topical application to the skin, particularly for the prevention or treatment of acne.

Acne is a follicular skin disease. The blackhead, which represents the initial tissue change in acne and is caused by the collision of keratinized cells within the sebaceous follicle, develops in several stages. Essentially, blackheads first develop as microcomedones, in which the follicular ostium begins to become distended by horny material and forms a keratin plug. The first visible tissue change is the closed blackhead or whitehead. The expansion of the follicular ostium by darkly pigmented horny material indicates the beginning of an open blackhead or blackhead. A subsequent rupture in the closed or open blackhead leads to the formation of secondary blackheads, which are generally larger and of varying shapes.

The building blocks of the horny structure of the blackheads are corneocytes (i.e. individual dead skin cells) held together by a cement-like substance of extracellular lipids. Closed and open blackheads develop into nodules and pustules, which are characteristic of inflammatory acne. Although there are several factors that appear to be crucial in the pathogenesis of acne, the formation of keratin plugs (i.e. hyperkeratosis accumulation) is the common denominator.

It is therefore obvious that a treatment aimed at preventing or removing such keratin plugs (keratolysis) reduces the pressure necessary for the formation of the blackhead and at the same time helps to remove existing blackheads (comedolysis).

Salicylic acid is a well-known, effective anti-acne agent that causes a reduction in the intercellular cohesion of corneocytes (see C. Huber et al., Arch. Derm. Res. 257, 293-297, 1977), thereby dissolving the existing keratin plugs and preventing the formation of new plugs. To best exert its keratolytic and comedolytic action, the ideal anti-acne composition should contain optimal concentrations of salicylic acid in the stratum corneum with low penetration through the skin and in the general circulation. Anti-acne compositions containing salicylic acid, benzoyl peroxide and surfactant are described in British Patent Specification GB-A-2 018 589.

According to the present invention, an effective anti-acne composition is provided in which substantial amounts of salicylic acid can be stored in the stratum corneum with minimal penetration through the skin. The resulting enhanced efficacy of salicylic acid, as evidenced by increased desquamation of corneocytes, occurs with less potential for irritation, drying of the skin and systemic side effects.

The anti-acne composition provided herein comprises a hydroalcoholic salicylic acid solution having a pH of 2 to 3.5 as an anti-acne active ingredient together with a specific anionic surfactant component. More specifically, the present invention provides a stable hydroalcoholic composition having a pH of 2 to 3.5 and containing from 0.2 to 5.0% by weight of salicylic acid and from 0.2 to 5.0% by weight of sodium methyl cocoyl taurate and/or sodium methyl oleoyl taurate as anionic surfactant component. Generally, a sufficient amount of a cosmetically acceptable alkaline component (i.e., an alkalizing agent) is included to provide and maintain the composition at a pH of 2.0 to 3.5.

As the alcohol component of the hydroalcoholic solvent, 10 to 60 wt% ethyl alcohol, measured as total C₂H₅OH content, is preferred, although an equal amount of isopropyl alcohol (C₃H₇OH) may also be used beneficially. As the aqueous component of the hydroalcoholic solvent, 30 to 80 wt% water is also required.

As previously stated, salicylic acid is a well-known active anti-acne ingredient. A listing of commercially available anti-acne products containing salicylic acid can be found in the report Physician's Desk Reference for Nonprescription Drugs, 7th edition, 1986, page 314.

The anionic surfactant component of the subject composition, i.e. the taurate surfactant component, is specifically directed to sodium methyl cocoyl taurate and sodium methyl oleoyl taurate, both of which are readily available from various suppliers, as described in The Cosmetic, Toiletry and Fragrance Association (CTFA) Cosmetic Ingredient Dictionary, 3rd edition, 1982, pages 286-287.

The pH of the subject composition of 2 to 3.5 can be achieved by using a suitable cosmetically acceptable primary or dual buffer system. In most cases, the resulting pH of the hydroalcoholic solution of salicylic acid will be slightly below or at the lower end of the indicated range and all that is required to adjust the pH to a desired higher value within the indicated range is the addition of an alkaline additive such as is generally used in cosmetic formulations for such purposes. Although sodium carbonate is preferred, other suitable alkalizing agents include potassium carbonate, sodium hydroxide, potassium hydroxide, triethanolamine and the like. If it appears necessary to change or adjust the pH to a lower value, a suitable acceptable acidifying agent such as citric acid may be used.

The following table lists the general and preferred amounts of the essential components of the subject composition: General Preferred Salicylic Acid Surfactant Taurate Alcohol Component Water pH Value

The compositions of the present invention have been found to be very effective in delivering and maintaining salicylic acid directly at the intended site of action, the stratum corneum, for optimal anti-acne efficacy with minimal penetration through the skin into the general circulation. Such surprising localization of action is attributed to the selective use of the above-mentioned surfactant taurate in the subject compositions. In contrast, other commonly used surfactants in the identical hydroalcoholic solution of salicylic acid (active ingredient) result in reduced localization in the stratum corneum and higher penetration of this active ingredient through the skin.

The following "Experimental Protocol" is followed to obtain the data given in the examples.

Test protocol A. Skin penetration/deposition:

Human skin samples are obtained at autopsy and maintained under sterile conditions until use. The diffusion cell setup and methodology used in skin penetration studies was previously described by S. Nacht et al., J. Am. Acad. Dermatol. 4(1):31-37, 1981; see also "Percutaneous Adsorption" edited by R. L. Bronaugh & H. I. Maibach, published by Marcel Dekker, Inc., N. Y., 1985, Chapter 29, "Artifical Membranes and Skin Permeability" by S. Nacht & D. Yeung. The diffusion cell consists of two parts: the lower chamber is made of Plexiglas and the upper part is made of Teflon. The skin sample is mounted so that the stratum corneum side is exposed to air and is held to the Teflon top with a rubber O-ring; a tight seal between the two chambers is achieved by tightening the screw set. The cell has an effective diffusion area of 5.08 cm2 and the dermis side of the skin is continuously bathed by filling the receptor chamber with 40 ml of isotonic saline. Appropriate mixing of the receptor phase is achieved with a magnetically driven Teflon-coated stir bar moved by a suitable motor located below the cell bath. The entire diffusion cell construction is immersed in a water bath maintained at 30ºC using a circulating water bath. The test formulation (0.25 ml) containing radiolabeled salicylic acid is applied to the upper surface of the epidermis. At hourly intervals for a seven-hour period, a one-milliliter sample of receptor fluid is taken and analyzed for radioactive content by a liquid scintillation counter (Packard Tri-Carb Model No. 460). Sample volumes are replaced with equal volumes of isotonic saline. All experiments are run in duplicate and the results are averaged. Each series of experiments is performed using donor skin from an identical skin site.

At the end of the seven-hour period, the skin sample is removed from the diffusion cell, trimmed of excess skin, and adhered to a glass plate using cyanoacrylate glue. The surface of the skin is wiped with a methanol-soaked swab to remove any product residue on the skin surface. Ten tape pulls are then taken in succession and the salicylic acid content per strip is determined. A more detailed discussion and description of tape pulls for measuring stratum corneum deposition is given by H. Schaefer et al. in "Skin Permeability", published by Springer-Verlag, NY, 1982, pages 554-58.

B. Keratolytic/desquamating efficacy

It has been reported in the literature that the effectiveness of salicylic acid in various formulations to increase skin desquamation in vivo can be assessed by quantifying the number of corneocytes removed from the skin surface (see D. Roberts et al., Br. J. Dermatol., 103, 191-196, 1980; and M.C. Christensen et al., J. Invest. Dermatol., 71:289:294, 1978). One such quantification of corneocytes removed uses an adhesive tape peel of the treated area after twice daily application (6-hour intervals) for seven days. The relative density of corneocytes per peel is correlatable to the number of corneocytes removed. The density of corneocytes removed is determined using a chromameter, which measures the light value (L*) of light reflected from the tape print when the print is placed on a black background. The higher the L* value, the greater the number of corneocytes on the tape print. Each formulation is applied to the inner forearm of a human subject at a dosage of 4 ul/cm2 twice daily (6 hours apart) for seven days. Approximately 6 hours after the last application, the treated area is stripped once with tape. The trial is performed on four subjects and the results are averaged. The results are reported as a percentage reduction in corneocytes removed compared to untreated skin. A reduction in corneocytes indicates more desquamation.

The subject compositions may also comprise optional additives such as antibacterial agents such as benzyl alcohol or methylparaben; antioxidants and preservatives such as ethylenediaminetetraacetic acid; astringents such as witch hazel; fragrances and sensates such as camphor or menthol; colorants and other cosmetically acceptable adjuvants commonly used in anti-acne compositions. Although the use of the surfactant taurate as the sole surfactant in the other surfactants may be incorporated, the non-ionic type being preferred over the anionic type because of the relative non-irritation of the former to the skin. Cationic surfactants, which are very irritating to the skin, are also unsuitable because of their marked sensitivity to hydrolysis at the low acidic pH of the subject compositions. Obviously, the choice and amount of any additional ingredient should be such that that ingredient does not adversely affect the beneficial properties of the taurate surfactant described above.

According to the present invention there is therefore provided an improved cosmetically acceptable hydroalcoholic composition having a pH of 2 to 3.5 and containing an antiacne effective amount of salicylic acid (0.2-5.0% w/w) together with an anionic surfactant, wherein the improvement comprises the use of sodium methyl cocoyl taurate or sodium methyl oleoyl taurate as said anionic surfactant (0.2-5.0% w/w).

The following examples serve to illustrate the present invention. Example 1 Basic formula: Salicylic acid Surfactant Sodium carbonate, up to pH 3 Water...to 100 %

Corresponding hydroalcoholic salicylic acid solutions are prepared by substituting the following anionic surfactants, identified by their names included in the CTFA, in the basic formula:

A = Sodium methyl cocoyl taurate

B = Sodium dodecylbenzylsulfonate

C = sodium C₁₂₋₁₅-alcohol sulfate

manufactured.

Example 2

The corresponding compositions of Example 1 are tested in vitro according to Test Protocol A and the resulting data demonstrate the improved localization of salicylic acid in the stratum corneum with Surfactant A. In contrast to Surfactants B and C, Surfactant A causes a significant increase in the deposition of salicylic acid in the stratum corneum, measured in micrograms (ug), along with a significant decrease in the rate of penetration through the stratum corneum, measured in ug/cm2/hr. The data for deposition presented in the table represent the average of two sets of ten consecutive tape peels and for penetration rate the average of two diffusion cells. Salicylic Acid Base Formula with Surfactant Deposit (ug) Penetration Rate (mg/cm² /h)

Example 3

In this example, the basic formula of Example 1 is modified by the indicated percentage of sodium methyl cocoyl taurate (surfactant A) and the resulting compositions are tested as in Example 2. Salicylic Acid % w/w of Surfactant A in the Base Formula Deposition (ug) Penetration Rate (ug/cm² /h)

Example 4

This example shows the effect of another anionic surfactant, sodium lauryl sulfate (surfactant D), Decrease in effectiveness. It also shows the relative effectiveness of the two surfactants taurates, sodium methyl cocoyl taurate (surfactant A) and sodium methyl oleoyl taurate (surfactant E). The basic formula of Example 1 is modified in a similar manner and tested according to Test Protocol A. Salicylic Acid % w/w of surfactant in the base formula Deposition (ug) Penetration rate (ug/cm² /h)

The results presented in the table show the similar effect between surfactants A and E, the two taurine surfactants of the present invention. On the other hand, the use of surfactant D, an anionic surfactant frequently used in cosmetic preparations, leads to a significant decrease in salicylic acid deposition in the stratum corneum and a significant increase in the penetration rate through the skin.

Example 5

In this example, sodium methyl cocoyl taurate (surfactant A) is compared with the anionic surfactant sodium lauryl sulfate (surfactant D) and the nonionic surfactant polysorbate 20 (surfactant F) at an equivalent concentration according to the previous examples. The results again show the clear superiority of the surfactant taurate. Salicylic Acid % w/w of surfactant in the base formula Deposition (ug) Penetration rate (ug/cm² /h)

Example 6

The three hydroalcoholic salicylic acid solutions containing surfactants A, B and C of Example 1 are tested in vivo according to test protocol B. The data on the percentage reduction in corneocytes shown in the table again demonstrate the clear superiority of surfactant A. Basic formula with surfactant % reduction in corneocytes

Example 7

This example illustrates the preferred compositions of the present invention containing additional optional ingredients. Each ingredient is identified by its generic chemical name or by its name incorporated in the CTFA. Ingredients 1. Salicylic acid 2. Na Methyl Cocoyl Taurate 3. Na Methyl Oleoyl Taurate 4. C₂H₅OH (95% ethanol) 5. Witch Hazel Distillate 6. Quaternium-22 7. Aloe Vera Gel 8. Allantoin 9. Anhydrous Na₂CO₃ 10. Aqueous Citric Acid 11. Menthol 12. Camphor 13. Flavor and Sensat Oils 14. Water ditto to 100%

In an appropriately sized vessel, add ingredients 4 and 5 while stirring at a moderate rate. Add ingredients 1, 11 and 12, ensuring that each ingredient is completely dissolved before the next addition. In a separate vessel, heat the surfactant taurate (ingredient 2 or 3) to 35-40ºC until clear and then add ingredient 13 while stirring until homogeneous. Add the taurate mixture to the alcoholic salicylic acid mixture while stirring. Slowly add ingredient 14 and then ingredients 6 and 7 and in compositions B and C, ingredient 8. Check the pH and adjust to about 3 by adding ingredients 9 (to raise the EP 0 pH) and 10 (to lower the pH) while stirring.

Claims (7)

1. A cosmetically acceptable composition for treating acne, which composition comprises: a) 0.2% to 5.0% by weight salicylic acid; b) 10 wt.% to 60 wt.% C₂H₅OH or C₃H₇OH; c) 30% to 80% by weight of water; and d) 0.2% to 5.0% by weight of sodium methyl cocoyl taurate or sodium methyl oleoyl taurate; the composition having a pH of 2 to 3.5. 2. A composition according to claim 1, wherein b) is C₂H₅OH and d) sodium methyl cocoyl taurate. 3. A composition according to claim 1, wherein b) is C₂H₅OH and d) sodium methyl oleoyl taurate. 4. A cosmetically acceptable composition for treating acne, which composition comprises: a) 0.5% to 2.5% by weight salicylic acid; b) 20 wt.% to 50 wt.% C₂H₅OH or C₃H₇OH: c) 50% to 75% by weight of water; and d) 0.2% to 2.5% by weight of sodium methyl cocoyl taurate or sodium methyl oleoyl taurate; the composition having a pH of 2 to 3.5. 5. A composition according to claim 4, wherein b) is C₂H₅OH and d) 0.7 wt% sodium methyl cocoyl taurate. 6. A composition according to claim 4, wherein b) is C₂H₅OH and d) 0.7 wt% sodium methyl oleoyl taurate. 7. A cosmetically acceptable composition for the treatment of acne, which composition comprises: Ingredients Salicylic acid Na-methylcocoyltaurate or Na-methyloleoyltaurate C₂H₅OH (95% ethanol) "Witch Hazel" distillate Quaternium-22 Aloe Vera gel Allantoin anhydrous Na₂CO₃ Citric acid, aqueous Menthol Camphor Aroma additive and sensually perceptible oils Water to 100%